TY - JOUR
T1 - Mutation in NSUN2, which encodes an RNA methyltransferase, causes autosomal-recessive intellectual disability
AU - Khan, Muzammil Ahmad
AU - Rafiq, Muhammad Arshad
AU - Noor, Abdul
AU - Hussain, Shobbir
AU - Flores, Joana V.
AU - Rupp, Verena
AU - Vincent, Akshita K.
AU - Malli, Roland
AU - Ali, Ghazanfar
AU - Khan, Falak Sher
AU - Ishak, Gisele E.
AU - Doherty, Dan
AU - Weksberg, Rosanna
AU - Ayub, Muhammad
AU - Windpassinger, Christian
AU - Ibrahim, Shahnaz
AU - Frye, Michaela
AU - Ansar, Muhammad
AU - Vincent, John B.
PY - 2012/5/4
Y1 - 2012/5/4
N2 - Causes of autosomal-recessive intellectual disability (ID) have, until very recently, been under researched because of the high degree of genetic heterogeneity. However, now that genome-wide approaches can be applied to single multiplex consanguineous families, the identification of genes harboring disease-causing mutations by autozygosity mapping is expanding rapidly. Here, we have mapped a disease locus in a consanguineous Pakistani family affected by ID and distal myopathy. We genotyped family members on genome-wide SNP microarrays and used the data to determine a single 2.5 Mb homozygosity-by-descent (HBD) locus in region 5p15.32-p15.31; we identified the missense change c.2035G>A (p.Gly679Arg) at a conserved residue within NSUN2. This gene encodes a methyltransferase that catalyzes formation of 5-methylcytosine at C34 of tRNA-leu(CAA) and plays a role in spindle assembly during mitosis as well as chromosome segregation. In mouse brains, we show that NSUN2 localizes to the nucleolus of Purkinje cells in the cerebellum. The effects of the mutation were confirmed by the transfection of wild-type and mutant constructs into cells and subsequent immunohistochemistry. We show that mutation to arginine at this residue causes NSUN2 to fail to localize within the nucleolus. The ID combined with a unique profile of comorbid features presented here makes this an important genetic discovery, and the involvement of NSUN2 highlights the role of RNA methyltransferase in human neurocognitive development.
AB - Causes of autosomal-recessive intellectual disability (ID) have, until very recently, been under researched because of the high degree of genetic heterogeneity. However, now that genome-wide approaches can be applied to single multiplex consanguineous families, the identification of genes harboring disease-causing mutations by autozygosity mapping is expanding rapidly. Here, we have mapped a disease locus in a consanguineous Pakistani family affected by ID and distal myopathy. We genotyped family members on genome-wide SNP microarrays and used the data to determine a single 2.5 Mb homozygosity-by-descent (HBD) locus in region 5p15.32-p15.31; we identified the missense change c.2035G>A (p.Gly679Arg) at a conserved residue within NSUN2. This gene encodes a methyltransferase that catalyzes formation of 5-methylcytosine at C34 of tRNA-leu(CAA) and plays a role in spindle assembly during mitosis as well as chromosome segregation. In mouse brains, we show that NSUN2 localizes to the nucleolus of Purkinje cells in the cerebellum. The effects of the mutation were confirmed by the transfection of wild-type and mutant constructs into cells and subsequent immunohistochemistry. We show that mutation to arginine at this residue causes NSUN2 to fail to localize within the nucleolus. The ID combined with a unique profile of comorbid features presented here makes this an important genetic discovery, and the involvement of NSUN2 highlights the role of RNA methyltransferase in human neurocognitive development.
UR - https://www.scopus.com/pages/publications/84860760092
U2 - 10.1016/j.ajhg.2012.03.023
DO - 10.1016/j.ajhg.2012.03.023
M3 - Article
C2 - 22541562
AN - SCOPUS:84860760092
SN - 0002-9297
VL - 90
SP - 856
EP - 863
JO - American Journal of Human Genetics
JF - American Journal of Human Genetics
IS - 5
ER -
